[No authors listed]
The specific role and mechanism of ferroptosis in the development of pancreatic cancer (PC) remain to be elucidated. The present study aimed to investigate the effects of the overexpression of the KAI1 gene on the ferroptosis of the human PC cell line MIA PaCaâ2. MIA PaCaâ2 cells infected with pCMVâKAI1 and selected by G418 and KAI1 protein were analyzed by western blotting. The MIA PaCaâ2 cells with a stable expression of the KAI1 gene were termed MIA PaCaâ2âKAI1. The proliferative capacities of MIA PaCaâ2 and MIA PaCaâ2âKAI1 cells were detected using Cell Counting Kitâ8. The reactive oxygen in the cells were compared by flow cytometry. The expressions of ferroportin (FPN) and glutathione peroxidase 4 (GPX4) protein were analyzed by western blotting. The KAI1 stable expression cell line was confirmed and relabeled as MIA PaCaâ2âKAI1. No significant differences in the proliferation of MIA PaCaâ2 and MIA PaCaâ2âKAI1 were identified. Following treatment with a ferroptosis blocker, the increase in the proliferation of MIA PaCaâ2âKAI1 (from 2.06±0.02 to 2.75±0.02) was more evident compared with MIA PaCaâ2 (from 2.94±0.02 to 2.95±0.02; P<0.05). The in MIA PaCaâ2âKAI1 was significantly higher compared with MIA PaCaâ2 (P<0.05). FPN and GPX4 protein demonstrated higher expression levels in MIA PaCaâ2âKAI1 compared with MIA PaCaâ2. Moreover, KAI1 exerted an obvious promotion effect on FPN expression. This study identified that the high expression of the KAI1 gene promoted the occurrence of ferroptosis in PC cells through its extensive effect on FPN and GPX4. KAI1âinduced ferroptosis did not significantly inhibit the proliferation of PC cells.
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